Publications by authors named "Melissa M Papargiris"
Background: Fresh patient specimens of castrate-resistant prostate cancer (CRPC) are invaluable for studying tumor heterogeneity and responses to current treatments. They can be used for primary patient-derived xenografts (PDXs) or serially transplantable PDXs, but only a small proportion of samples grow successfully. To improve the efficiency and quality of PDXs, we investigated the factors that determine the initial engraftment of patient tissues derived from TURP specimens.
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- Most prostate cancer cases are now diagnosed as moderate-grade localized disease, which is challenging to study in the lab due to growth difficulties.
- A new system has been developed to xenograft human prostate cancer tissue into immunodeficient mice, allowing researchers to study interactions between different cell types in the tumors.
- This method enables long-term growth of grafts for testing new treatments, ultimately aiming to personalize therapy for individual prostate cancer patients.
Basic and translational (or preclinical) prostate cancer research has traditionally been conducted with a limited repertoire of immortalized cell lines, which have homogeneous phenotypes and have adapted to long-term tissue culture. Primary cell culture provides a model system that allows a broader spectrum of cell types from a greater number of patients to be studied, in the absence of artificially induced genetic mutations. Nevertheless, primary prostate epithelial cell culture can be technically challenging, even for laboratories experienced in immortalized cell culture.
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